Replication of GWAS-identified neuroblastoma risk loci strengthens the role of BARD1 and affirms the cumulative effect of genetic variations on disease susceptibility

Capasso, Mario; Diskin, Sharon J.; Totaro, Francesca; Longo, Luca; Mariano, Marilena De; Russo, Roberta; Cimmino, Flora; Hákonarson, Hákon; Tonini, Gian Paolo; Devoto, Marcella; Maris, John M.; Iolascon, Achille

doi:10.1093/carcin/bgs380

Cited by 97 publications

(132 citation statements)

References 20 publications

Supporting

Mentioning

125

Contrasting

Order By: Relevance

“…This study indicated that three SNPs in the FLJ22536 gene mapping to chromosome 6p22 were significantly associated with neuroblastoma susceptibility [8]. The association of 6p22 locus with neuroblastoma susceptibility has been replicated in subsequent studies using diverse populations, including African-Americans [13] and Italians [14].…”

Section: Introductionmentioning

confidence: 63%

“…Latorre et al [13] investigated the association of all these three polymorphisms in 390 African-American neuroblastoma patients and 2500 healthy controls; however, they failed to prove the association with altered neuroblastoma susceptibility for any of three SNPs. Capasso et al [14] attempted to test the association between two polymorphisms (rs6939340 A>G and rs4712653 T>C) and neuroblastoma susceptibility with 370 cases and 809 controls in an Italian population; they confirmed a significant association between both of these two polymorphisms and neuroblastoma susceptibility. As far as we knew, no validation study was performed among Asians except ours; we found that all of these three SNPs were associated with decreased neuroblastoma susceptibility in the current study.…”

Section: Discussionmentioning

confidence: 95%

“…They found that three polymorphisms located at the 6p22 and within the predicted gene FLJ22536 were associated with neuroblastoma susceptibility, and they also validated these results using additional 720 patients and 2128 control subjects. Later on, two validation studies were performed to verify the association between these FLJ22536 genetic variants and neuroblastoma risk for African-Americans [13] and Italian population [14]. Latorre et al [13] investigated the association of all these three polymorphisms in 390 African-American neuroblastoma patients and 2500 healthy controls; however, they failed to prove the association with altered neuroblastoma susceptibility for any of three SNPs.…”

Section: Discussionmentioning

confidence: 99%

“…Although the association with rs6939340 A>G, rs4712653 T>C, and rs9295536 C>A polymorphisms in the FLJ22536 gene has been replicated in previous studies involving African-Americans [13] and European descents [14], it remains unclear whether these polymorphisms also confer neuroblastoma susceptibility in Asians. Given the possible variations in minor allele frequency (MAF) and pattern of linkage disequilibrium across races, genetic susceptibility to neuroblastoma may largely differ between Asians and Caucasians.…”

Section: Introductionmentioning

confidence: 96%

See 3 more Smart Citations

Evaluation of GWAS-identified SNPs at 6p22 with neuroblastoma susceptibility in a Chinese population

Zhang

Zou

et al. 2015

Tumor Biol.

View full text Add to dashboard Cite

Previous genome-wide association studies (GWASs) have reported that three single nucleotide polymorphisms (SNPs) (rs6939340 A>G, rs4712653 T>C, and rs9295536 C>A) located at 6p22 locus were associated with neuroblastoma susceptibility for Caucasian descent. We conducted this hospital-based case-control study with 201 neuroblastoma patients and 531 controls to investigate the association between these three SNPs in the FLJ22536 gene with neuroblastoma susceptibility in the Chinese Han population. The odds ratio (OR) and 95 % confidence interval (CI) were calculated to estimate the strength of the association using unconditional logistic regression model. We found that the rs6939340 A allele carriers were associated with significantly decreased neuroblastoma susceptibility (AG vs. GG: adjusted OR = 0.54, 95 % CI = 0.38-0.77; AA vs. GG: adjusted OR = 0.49, 95 % CI = 0.25-0.93; and AA/AG vs. GG: adjusted OR = 0.53, 95 % CI = 0.38-0.74) after adjustment for age and gender. The protective association between variant allele and neuroblastoma susceptibility was also observed for the rs4712653 and rs9295536 polymorphisms. Moreover, we found that subjects carrying one or more protective genotypes had a much lower neuroblastoma susceptibility than non-carriers (adjusted OR = 0.60, 95 % CI = 0.43-0.83). Our study verified that the associations between all of the three SNPs in the 6p22 locus are associated with neuroblastoma susceptibility in the Chinese subjects. Further prospective multicenter studies with different ethnicities and larger sample size are needed to validate our findings.

show abstract

Section: Introductionmentioning

confidence: 63%

Section: Discussionmentioning

confidence: 95%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 96%

See 2 more Smart Citations

Evaluation of GWAS-identified SNPs at 6p22 with neuroblastoma susceptibility in a Chinese population

Zhang

Zou

et al. 2015

Tumor Biol.

View full text Add to dashboard Cite

show abstract

“…Familial neuroblastoma is rare (approximately 1%), and most of these cases harbour germline mutations in ALK 1. In contrast, the genetic bases of sporadic neuroblastoma remain largely unknown 2, 3. Through a genomewide association study (GWAS) of sporadic neuroblastoma, we have reported common single nucleotide polymorphisms (SNPs) associated with neuroblastoma susceptibility at CASC15 4, BARD1 5, LMO1 6, DUSP12 7, HSD17B12 7, DDX4/IL31RA 7, HACE1 8 and LIN28B 8 loci.…”

Section: Introductionmentioning

confidence: 99%

The functional variant rs34330 of CDKN1B is associated with risk of neuroblastoma

Capasso

McDaniel

Cimmino

et al. 2017

J Cellular Molecular Medi

Self Cite

View full text Add to dashboard Cite

The genetic aetiology of sporadic neuroblastoma is still largely unknown. We have identified diverse neuroblastoma susceptibility loci by genomewide association studies (GWASs); however, additional SNPs that likely contribute to neuroblastoma susceptibility prompted this investigation for identification of additional variants that are likely hidden among signals discarded by the multiple testing corrections used in the analysis of genomewide data. There is evidence suggesting the CDKN1B, coding for the cycle inhibitor p27Kip1, is involved in neuroblastoma. We thus assess whether genetic variants of CDKN1B are associated with neuroblastoma. We imputed all possible genotypes across CDKN1B locus on a discovery case series of 2101 neuroblastoma patients and 4202 genetically matched controls of European ancestry. The most significantly associated rs34330 was analysed in an independent Italian cohort of 311 cases and 709 controls. In vitro functional analysis was carried out in HEK293T and in neuroblastoma cell line SHEP‐2, both transfected with pGL3‐CDKN1B‐CC or pGL3‐CDKN1B‐TT constructs. We identified an association of the rs34330 T allele (‐79C/T) with the neuroblastoma risk (Pcombined = 0.002; OR = 1.17). The risk allele (T) of this single nucleotide polymorphism led to a lower transcription rate in cells transfected with a luciferase reporter driven by the polymorphic p27Kip1 promoter (P < 0.05). Three independent sets of neuroblastoma tumours carrying ‐79TT genotype showed a tendency towards lower CDKN1B mRNA levels. Our study shows that a functional variant, associated with a reduced CDKN1B gene transcription, influences neuroblastoma susceptibility.

show abstract

Advances in the translational genomics of neuroblastoma: From improving risk stratification and revealing novel biology to identifying actionable genomic alterations

Bosse

Maris

2015

Cancer

Self Cite

183

161

View full text Add to dashboard Cite

Neuroblastoma is an embryonal malignancy that commonly affects young children and is remarkably heterogenous in its malignant potential. Recently, the genetic basis of neuroblastoma has come into focus, which has catalyzed not only a more comprehensive understanding of neuroblastoma tumorigenesis, but has also revealed novel oncogenic vulnerabilities that are being leveraged therapeutically. Neuroblastoma is a model pediatric solid tumor in its use of recurrent genomic alterations, such as high-level MYCN amplification, for risk stratification. Given the relative paucity of recurrent activating somatic point mutations or gene fusions in primary neuroblastoma tumors studied at initial diagnosis, innovative treatment approaches beyond small molecules targeting mutated or dysregulated kinases will be required moving forward to achieve noticeable improvements in overall patient survival. However, the clonally acquired, oncogenic aberrations in relapsed neuroblastomas are currently being defined and may offer an opportunity to improve patient outcomes with molecularly targeted therapy directed towards aberrantly regulated pathways in relapsed disease. This review will summarize the current state of knowledge of neuroblastoma genetics and genomics, highlighting the improved prognostication and potential therapeutic opportunities that have arisen from recent advances in understanding germline predisposition, recurrent segmental chromosomal alterations, somatic point mutations and translocations, and clonal evolution in relapsed neuroblastoma.

show abstract

Replication of GWAS-identified neuroblastoma risk loci strengthens the role of BARD1 and affirms the cumulative effect of genetic variations on disease susceptibility

Cited by 97 publications

References 20 publications

Evaluation of GWAS-identified SNPs at 6p22 with neuroblastoma susceptibility in a Chinese population

Evaluation of GWAS-identified SNPs at 6p22 with neuroblastoma susceptibility in a Chinese population

The functional variant rs34330 of CDKN1B is associated with risk of neuroblastoma

Advances in the translational genomics of neuroblastoma: From improving risk stratification and revealing novel biology to identifying actionable genomic alterations

Contact Info

Product

Resources

About